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JPH0351688B2 - - Google Patents

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Publication number
JPH0351688B2
JPH0351688B2 JP60252590A JP25259085A JPH0351688B2 JP H0351688 B2 JPH0351688 B2 JP H0351688B2 JP 60252590 A JP60252590 A JP 60252590A JP 25259085 A JP25259085 A JP 25259085A JP H0351688 B2 JPH0351688 B2 JP H0351688B2
Authority
JP
Japan
Prior art keywords
ulcer
pyrimidine
hexahydro
oxo
dimethyl
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Lifetime
Application number
JP60252590A
Other languages
Japanese (ja)
Other versions
JPS61171420A (en
Inventor
Mesuzarosu Zorutan
Kunooru Yozusefu
Herumekuzu Isutoban
Suzentomikuroshi Peetaa
Horubasu Agunesu
Basubari Ne Deiiaaru Deburekujii Rere
Kobakusu Gabooru
Giiresu Kurara
Biragu Sandooru
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
KINOIN GIOGISUZERU ESU BEGIESUZECHI TERUMEKEKU GIARA RUTO
Original Assignee
KINOIN GIOGISUZERU ESU BEGIESUZECHI TERUMEKEKU GIARA RUTO
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by KINOIN GIOGISUZERU ESU BEGIESUZECHI TERUMEKEKU GIARA RUTO filed Critical KINOIN GIOGISUZERU ESU BEGIESUZECHI TERUMEKEKU GIARA RUTO
Publication of JPS61171420A publication Critical patent/JPS61171420A/en
Publication of JPH0351688B2 publication Critical patent/JPH0351688B2/ja
Granted legal-status Critical Current

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Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/33Heterocyclic compounds
    • A61K31/395Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
    • A61K31/495Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with two or more nitrogen atoms as the only ring heteroatoms, e.g. piperazine or tetrazines
    • A61K31/505Pyrimidines; Hydrogenated pyrimidines, e.g. trimethoprim
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P1/00Drugs for disorders of the alimentary tract or the digestive system
    • A61P1/04Drugs for disorders of the alimentary tract or the digestive system for ulcers, gastritis or reflux esophagitis, e.g. antacids, inhibitors of acid secretion, mucosal protectants

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  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • Veterinary Medicine (AREA)
  • Public Health (AREA)
  • Medicinal Chemistry (AREA)
  • General Health & Medical Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Epidemiology (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Organic Chemistry (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • General Chemical & Material Sciences (AREA)
  • Engineering & Computer Science (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Nitrogen Condensed Heterocyclic Rings (AREA)
  • Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)

Abstract

The invention relates to a process for the restoration and prevention of gastriontestinal injuries, which comprises treating a patient with an effective dose of racemic or optically active 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-4H-pyrimi- do/1,2-a/pyrimidine-3-carboxamide.

Description

【発明の詳现な説明】 産業䞊の利甚分野 本発明は、有効成分ずしお、ラセミ䜓の又は光
孊的掻性の−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリ
ド−ピリミゞン−−カルボキシア
ミドを含有する、人間や動物の朰瘍を予防し、治
療するための医薬甚薬剀に関するものである。 埓来の技術 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドは、
鎮痛及び消炎䜜甚を有するこずは知られおいる
〔英囜特蚱明现曞No.1583896「アルツナむミツテ
ルフオルシナング」Arzneimittelforschung
297661979〕。 重い傷害やも぀ずひどい堎合には、生呜を脅か
す胃腞障害さえ、消炎剀によ぀お誘発されるこず
も知られおいる〔「トレンズ・むン・フアルム・
゜サむテ」Trends in Pharm. Sci.156
1984〕。 最も䞀般に、広く甚いられおいる消炎薬品の副
䜜甚の頻床を衚に瀺す。 これらの副䜜甚が、胃腞系統の限られた範囲に
及がすのみであるので、これらの胃腞障害は、他
の薬品で郚分的にのみ治療しうる〔「バヌガヌ
ズ・メゞカル・ケミストリむ」Burgers
Medicinal Chemistry第版、第巻、835−
853ペヌゞ及び第巻、361−406ペヌゞ及び507−
534ペヌゞ、ゞペン・りむレむ・アンド・サンズ
John Wiley and Sons1979−1981幎発行〕。 発明が解決しようずする問題点 本発明の目的は化孊的な、又は倖因性もしくは
内因性の薬剀によ぀お生じた朰瘍に察する保護ず
回埩を胃腞系統党䜓に䞎えるために、−ゞ
メチル−−オキ゜−9a
−ヘキサヒドロ−4H−ピリド−ピ
リミゞン−−カルボキシアミドを含有する医薬
甚薬剀を提䟛するこずにある。䞊蚘化合物は日
あたり10〜1000mgの量で投䞎される。 問題点を解決するための手段 その化合物の有効性を、140〜170の重さの
雄、雌のスプレヌグ−ダりレむSprague−
DawleyCFYのラツトをそれぞれ甚いお、むン
ドメタシンにより、100mlの溶液に濃塩酞mlを
含む゚タノヌルにより、及び0.6モル濃床の塩酞
により誘起された傷害に関しお研究した。各矀
は、10匹からな぀おいた。実隓を始める前は、そ
の動物は食物ず氎を無制限に䞎えながら、21℃で
日間ある郚屋の䞭での環境に順応させた。その
実隓の24時間前は、動物には氎のみを䞎えた。 第䞀察照矀の動物には朰瘍を起させる薬剀ずし
おむンドメタシンの20mgKg䜓重以䞋mg
Kgず略す、又ぱタノヌル性塩酞0.5ml、又は、
0.6モル濃床の塩酞mlを経口により䞎えた。 第二察照矀の動物には、メンドメタシンを䞎え
お30分経お、シメチゞンの12.5mgKgを皮䞋によ
り、又ぱタノヌル性塩酞を䞎える40分前に50
mgKgのシメチゞンを経口により、又は0.6モル
濃床の塩酞を䞎える時間前に、シメチゞンの50
mgKgを経口により䞎えた。 第䞉察照矀の動物には、むンドメタシンを経口
服甚させお30分経お0.5mgKgのアストロピンを
皮䞋により、又ぱタノヌル性塩酞を䞎える20分
前にアストロピンの1.0mgKgを皮䞋により、又
は0.6モル濃床の塩酞を䞎える30分前にアストロ
ピンの1.0mgKgを皮䞋により䞎えた。 第四矀の動物には、むンドメタシンず同時に
−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドの50
mgKgを経口により、又ぱタノヌル性塩酞を䞎
える40分前に−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−
ピリド−−ピリミゞン−−カルボ
キシアミドの50mgKgを経口により、又は0.6モ
ル濃床の塩酞を投䞎する時間前に、−ゞ
メチル−−オキ゜−9a
−ヘキサヒドロ−4H−ピリド−−ピ
リミゞン−−カルボキシアミドの50mgKgを経
口により䞎えた。 その結果を、傷害を起こす薬剀の投䞎埌すなわ
ちむンドメタシンを投䞎しお時間埌に、゚タノ
ヌル性塩酞を䞎えお時間埌に、そしお0.6モル
濃床塩酞を䞎えお時間埌に、それぞれ評䟡し
た。 銖を切぀お埌、動物の胃を、倧きい湟曲に沿぀
お切開した。むンドメタシンの堎合は、胃の粘膜
の傷害は、アダムス法〔アルシヌブ アンテルナ
シペナル ドり フアルマコデむナミヌArch.
Int.Pharmacudyn.1471131964〕を甚いお
枬定した。その倉化を頻床ず重床によ぀お次の通
り分類した。 完党な粘膜  点状の出血  〜個の小朰瘍  倚数の小朰瘍又は個の倧朰瘍  倚数の倧朰瘍  ゚タノヌル性塩酞、0.6モル濃床の塩酞の各堎
合には、その倉化を、朰瘍の数、重床、頻床に埓
぀お評䟡した。朰瘍圢成の重床は、次の通り採点
した。 完党な粘膜  〜mmの長さの朰瘍かびらん  〜mmの長さの朰瘍  〜mmの長さの朰瘍  mmより長い朰瘍  mmより長い厚い朰瘍  衚に瀺した結果は、−ゞメチル−−
オク゜−9a−ヘキサヒド
ロ−4H−ピリド−ピリミゞン−
−カルボキシアミドは、䞉぀の朰瘍化剀すべおに
察しお効果を有するこずが立蚌され、䞀方シメチ
ゞン及びアストロピンは、むンドメタシンによる
朰瘍の圢成のみを抑制したこずを䟋瀺しおいる。 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドは、
衚に瀺した実隓結果によ぀お䟋瀺したように、
急性の治療のみでなく効果があるこずが立蚌され
た。 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドを、
日間続けお経口により、50mgKgの服甚量を投
䞎したずいうこずを陀けば、これらの実隓のやり
方は、急性の実隓の堎合ず同様であ぀た。傷害を
起させる薬剀゚タノヌル性塩酞、又は0.6モル
濃床の塩酞を日目に投䞎し、その実隓を、急
性の実隓で述べたずの同様に評䟡した。 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドは、
゚タノヌル性塩酞か又は0.6モル濃床の塩酞によ
぀お生じたも぀ず重倧な倉化の進展に察しお保護
効果を䞎えるこずができた。 朰瘍の頻床のみならずその数ず重床も枛少し
た。朰瘍化は、察照矀の各動物で発生した。䞀方
−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドで治
療された各動物ではそれ皋重くない朰瘍が60ある
いは80の割合で芳察されたのみである。 保護䜜甚ず進展した傷害の回埩が胃の䞭ばかり
でなく、胃腞系統の他の郚分においおも同様に、
−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドによ
぀お䞎えられた。腞での朰瘍圢成䞊の効果を、10
匹のスプレヌグ−ダりレむCFYのねずみの矀で、
シメチゞン及びアストロピンの堎合ず比范しお研
究した。胃粘膜の傷害を抑制する化合物が、腞の
朰瘍化を抑制するこずができるか吊かを知るこず
も、たた非垞に重芁なこずである。胃粘膜の傷害
が、抑制されるのみである堎合には、その時は、
腞の瘍は有孔ずなる〔ブリテむツシナ ゞダヌナ
ル オブ パヌマ コロゞむBritish J.Pham.
67331979〕。 䞊述した実隓ず同様に、むンドメタシンを朰瘍
化剀ずしお甚いた。 研究䞭の化合物シメチゞン、アストロピン、
−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミドのそ
れぞれを日間連続しおその動物に投䞎し、䞀方
朰瘍化剀むンドメタシンを、日目に䞀床䞎
えた。実隓䞭は、動物には無制限に食物ず氎を䞎
えた。日経぀た埌に動物を殺し、腹郚を切開し
お、胃腞系統の傷害をツモリ法〔ゞダヌナル オ
ブ パヌマ コロゞむD.J.Pharm.D.659
−6601980〕を甚いお枬定した。その朰瘍は、
次の通り朰瘍化指数によ぀お採点した。 完党な粘膜  〜個の小朰瘍又はびらん  〜個の朰瘍又はびらん  個より倚い朰瘍又は〜個の有孔朰瘍  倚くの有孔朰瘍  死亡した動物の芳察や、幜門から盲腞たでの小
腞の長さの芳察の倖に、動物の䜓重や腹氎化の頻
床もたた枬定した。 第䞀察照矀は、いかなる保護剀も朰瘍化剀も䞎
えなか぀た。第二察照矀は、朰瘍化剀、すなわち
むンドメタシンのみを䞎えた。第䞉察照矀は朰瘍
化剀ずシメチゞンを䞎えた。䞀方第四察照矀は、
朰瘍化剀の倖にアストロピンを䞎えた。第五察照
矀は、日間−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−
ピリド−ピリミゞン−−カルボキ
シアミドを䞎えた。 第六矀は、日間朰瘍化剀の倖に−ゞメ
チル−−オキ゜−9a−
ヘキサヒドロ−4H−ピリド−ピリ
ミゞン−−カルボキシアミドを䞎えた。これら
の実隓の結果を衚に芁玄する。−ゞメチ
ル−−オキ゜−9a−ヘ
キサヒドロ−4H−ピリド−ピリミ
ゞン−−カルボキシアミドは、調査されたすべ
おの倉数に関しお保護的効果を䞎えうるだけであ
るず結論づけられる。アストロピンの保護的効果
はそれ皋明癜ではなか぀た。 曎に、−ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリ
ド−ピリミゞン−−カルボキシア
ミドの保護䜜甚を、急性及び日間の実隓で、塩
酞を含たない玔゚タノヌルによ぀お誘起された胃
朰瘍の圢成に぀いお研究した。その結果を衚に
瀺す。 急性の実隓では、−ゞメチル−−オキ
゜−9a−ヘキサヒドロ−
4H−ピリド−ピリミゞン−−カ
ルボキシアミドを、0.5mlの゚タノヌルの経口投
䞎の40分前にスプレヌグ−ダりレむCFYのねず
みに経口投䞎した。 続けお日間の実隓䞭には、動物は、−
ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド−
ビリミゞン−−カルボキシアミドを続けお日
間経口により䞎え、日間には、−ゞメチ
ル−−オキ゜−9a−ヘ
キサ−ヒドロ−4H−ピリド−ピリ
ミゞン−−カルボキシアミドを䞎えたのに続い
お40分経お0.5mlの゚タノヌルを経口により䞎え
た。朰瘍抑制䜜甚を、朰瘍化剀を投䞎しお時間
埌に、䞡方の実隓で、枬定した。朰瘍圢成の重床
は、次の通り採点した。 完党な粘膜  〜mmの長さの朰瘍又はびらん  〜mmの長さの朰瘍  〜mmの長さの朰瘍  mmより長い朰瘍  mmより長い厚い朰瘍  衚に瀺すように、−ゞメチル−−オ
キ゜−9a−ヘキサヒドロ
−4H−ピリド−ピリミゞン−−
カルボキシアミドが日間の治療ばかりでなく急
性実隓においおも、゚タノヌルによる胃朰瘍圢成
を抑制した。 䜜 甚 衚〜に芁玄するず、−ゞメチル−
−オキ゜−9a−ヘキサヒ
ドロ−4H−ピリド−ピリミゞン−
−カルボキシアミドは、胃腞系統党䜓に保護及
び予防効果を䞎えるただ䞀぀の薬剀であ぀たこず
は明らかであるが、䞀方察照ずしお甚いたシメチ
ゞン及びアストロピンの䞡方の圱響は、傷害を起
こす薬剀いかんによるものずしお胃の保護に関䞎
したにすぎなか぀た。 発明の効果 本発明によれば、−ゞメチル−−オキ
゜−9a−ヘキサヒドロ−
4H−ピリド−ピリミゞン−−カ
ルボキシアミドは、予防法か治療法のいずれかを
甚いるこずによ぀お、化孊的な、又は他の倖因性
及び内因性の薬剀により生じた傷害に察しお、胃
腞系党䜓に保護䜜甚ず回埩を䞎えるものである。 その治療は、凊方の皮類いかんによ぀お有効成
分の玄10〜1000mgを含む錠剀、カプセル、糖衣
錠、坐薬、泚射のような䞀般に甚いられおいる補
薬組成物によ぀お実斜される。 日に䞀床か又は分割した服甚量を甚いるか
は、患者の状態や幎霢、傷害の重さ、䜿甚方法に
よ぀お倉わる。 毎日の経口服甚量は、100〜1000mg間で倉わる。 進展した傷害の重さによ぀お、非経口、特に皮
䞋や、皮膚内郚や、静脈による薬物治療もたた甚
いられる。 毎日の静脈による服甚量は10〜400mg間で倉わ
る。皮䞋投䞎の堎合、20〜800mgの服甚量が䞎え
られる。 【衚】 【衚】 【衚】 【衚】 【衚】 【衚】 【衚】 実斜䟋 本発明の実斜䟋を以䞋の非限定䟋によ぀お詳现
に瀺す。 䟋  有効成分の100mgをそれぞれ含む錠剀の調補 −ゞメチルヌ−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミド1000
ず乳糖300を含む混合物をふるいにかけ、均
䞀にし、それからこの粉状の混合物をれラチ
ン氎溶液200mlで湿最した。也燥、再粒状化埌、
その粒状物を、ステアリンリン酞マグネシりム塩
20、滑石40及びポテトデンプン40を含む粉
状混合物ずで均䞀にし、それから錠剀に圧瞮し
た。 䟋  有効成分の200mgをそれぞれ含む錠剀の調補 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミド2000
ずポテトデンプン600を含む混合物をふるい
にかけ、均䞀にし、それからこの粉状混合物を、
れラチン氎溶液300mlで湿最した。也燥、再
粒状化埌、その粒状物を滑石40、ステアリン酞
マグネシりム塩30、及びポテトデンプン30を
含む粉状混合物ずで均䞀にし、それから錠剀に圧
瞮した。 䟋  有効成分の300mgを各々含む錠剀の調補 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミド3000
ずポテトデンプン300を含む混合物をふるい
にかけ、均䞀にし、それらこの粉状混合物を500
mlのれラチン氎溶液で湿最した。也燥、再粒
状化埌、その粒状物を滑石120、ステアリン酞
マグネシりム塩50及びポテトデンプン30を含
む粉状混合物ずで均䞀にし、それから錠剀に圧瞮
した。 䟋  有効成分の100mg、200mg、300mgの各量を各含
む糖衣錠の調補 100mg、200mg、300mgの各量の−ゞメチ
ル−−オキ゜−9a−ヘ
キサヒドロ−4H−ピリド−ピリミ
ゞン−−カルボキシアミドを含む錠剀を被芆す
るのに顔料懞濁液を甚いた。 滑石64ず二酞化チタン50を含む现粉混合物
を、む゜プロパノヌル268ずで均䞀にした。氎
12䞭に氎溶性染料ずカヌボワツクス6000
を含む有色氎溶液を調補し、䞊蚘で調補した
懞濁液ず混合した。こうしお埗られた䞊薬甚の懞
濁液を1000個の錠剀の衚面を被膜するのに甚い
た。 䟋  泚射溶液ml100の調補ml100
 −ゞメチル−−オキ゜−
9a−ヘキサヒドロ−4H−ピリド
−ピリミゞン−−カルボキシアミド1000
をの容量のメスフラスコで秀量し、泚射甚
に甚いる氎に溶解した。泚射甚の氎で20に完党
に溶解埌぀くり䞊げ、ガラスフむルタヌを通しお
ろ過し、透明にした。 埗られた溶液を、120℃、30分間殺菌したml
容積のガラスびんに充おんした。 䟋  有効成分の200mgを含む坐薬の調補 コロむド状氎酞化ケむ玠物50を坐薬基剀2250
に分散させ、40〜45℃で液化アデツプス固盞
線させた。10Όの粒子埄をも぀た−ゞメ
チル−−オキ゜−9a−
ヘキサヒドロ−4H−ピリド−ピリ
ミゞンの200の量を、少量の液化坐薬基剀ず共
に絶えずかきたぜながら懞濁させた。 その懞濁物を必芁な補充量の固䜓脂肪の液化物
ず混合し、平均重量2.5の1000個の坐薬を埗る
ために目盛を぀けた坐薬鋳型に充おんした。 䟋  有効成分の100mgmlを含む也燥シロツプの
調補 シペ糖156ずカカオの粉末240を含む均䞀混
合物に、保存剀ずしお、メチル−−ヒドロオキ
シ安息銙酞塩0.25及びプロピル−−ヒドロオ
キシ安息酞塩0.35を、芳銙化剀ずしおバニリン
0.40を加えた。その埌−ゞメチル−−
オキ゜−9a−ヘキサヒド
ロ−4H−ピリド−ピリミゞン−
−カルボキシアミドの20をこの粉状混合物に察
し秀量し、再床均䞀にしおから、ふるいにかけ
た。 䜿甚前、この混合物を氎で1000にたで満たし
た。 Detailed Description of the Invention (Industrial Application Field) The present invention provides racemic or optically active 1,6-dimethyl-4-oxo-1,
Related to pharmaceutical agents for preventing and treating ulcers in humans and animals, containing 6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide It is. (Prior art) 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide is
It is known to have analgesic and anti-inflammatory effects [British Patent Specification No. 1583896; "Arzneimittelforschung"]
29, 766 (1979)]. It is also known that in severe injuries and in severe cases, even life-threatening gastrointestinal disorders can be induced by anti-inflammatory drugs.
Trends in Pharm. Sci. 5 , 156
(1984)]. Table 1 shows the frequency of side effects of the most commonly used anti-inflammatory drugs. Because these side effects affect only a limited area of the gastrointestinal system, these gastrointestinal disorders can only be partially treated with other drugs (Burgers Medical Chemistry).
Medicinal Chemistry), 4th edition, Volume 2, 835-
Pages 853 and Volume 3, pages 361-406 and 507-
534 pages, published by John Wiley and Sons 1979-1981]. SUMMARY OF THE INVENTION It is an object of the present invention to provide the entire gastrointestinal system with protection and recovery from ulcers caused by chemical, exogenous or endogenous agents. Dimethyl-4-oxo-1,6,7,8,9,9a
An object of the present invention is to provide a pharmaceutical agent containing -hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide. The above compounds are administered in amounts of 10 to 1000 mg per day. (Means for Solving the Problem) The effectiveness of the compound was tested in male and female Sprague-Dawleys weighing 140-170 g.
Dawley CFY rats were studied for the injury induced by indomethacin, by ethanol containing 2 ml of concentrated hydrochloric acid in 100 ml of solution, and by 0.6 molar hydrochloric acid. Each group consisted of 10 animals. Before starting the experiment, the animals were acclimatized in a room at 21°C for 4 days with ad libitum access to food and water. Animals were given water only for 24 hours before the experiment. Animals in the first control group received 20 mg/Kg (body weight) (hereinafter mg/kg) of indomethacin as a drug that causes ulcers.
Kg), or 0.5ml of ethanolic hydrochloric acid, or
1 ml of 0.6 molar hydrochloric acid was given orally. Animals in the second control group received either 12.5 mg/Kg of cimetidine subcutaneously 30 minutes after receiving mendomethacin or 50 minutes before receiving ethanolic hydrochloric acid.
mg/Kg cimetidine orally or 50 mg/Kg of cimetidine 1 hour before giving 0.6 molar hydrochloric acid.
mg/Kg was given orally. Animals in the third control group received either 0.5 mg/Kg of atropine subcutaneously 30 minutes after receiving indomethacin orally, or 1.0 mg/Kg of atropine subcutaneously 20 minutes before receiving ethanolic hydrochloric acid. Alternatively, 1.0 mg/Kg of astropine was given subcutaneously 30 minutes before giving 0.6 molar hydrochloric acid. Group 4 of animals received 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) pyrimidine-3-carboxamide 50
mg/Kg orally or 40 minutes before giving ethanolic hydrochloric acid.
1,6,7,8,9,9a-hexahydro-4H-
50 mg/Kg of pyrido-(1,2-a)pyrimidine-3-carboxamide orally or 1 hour before administration of 0.6 molar hydrochloric acid, 1,6-dimethyl-4-oxo-1,6 ,7,8,9,9a
50 mg/Kg of -hexahydro-4H-pyrido-(1,2-a)pyrimidine-3-carboxamide was given orally. The results were evaluated after administration of the injurious agent, ie, 4 hours after administration of indomethacin, 2 hours after administration of ethanolic hydrochloric acid, and 1 hour after administration of 0.6 molar hydrochloric acid. After decapitation, the animal's stomach was incised along a large curve. In the case of indomethacin, injury to the gastric mucosa is treated using the Adams method [Arch.
Int.Pharmacudyn.) 147, 113 (1964)]. The changes were classified as follows according to frequency and severity. Intact mucous membrane 0 Petechial bleeding 1 1 to 5 small ulcers 2 Many small ulcers or 1 large ulcer 3 Many large ulcers 4 Changes in each case of ethanolic hydrochloric acid and 0.6 molar hydrochloric acid were evaluated according to number, severity, and frequency of ulcers. The severity of ulceration was scored as follows. Complete mucous membrane 0 Ulcers or erosions with a length of 1-2 mm 1 Ulcers with a length of 2-3 mm 2 Ulcers with a length of 3-4 mm 3 Ulcers longer than 4 mm 4 Thick ulcers longer than 4 mm 5 Results shown in Table 2 is 1,6-dimethyl-4-
Oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3
- Carboxamides were demonstrated to be effective against all three ulcerating agents, while cimetidine and atropine were exemplified to inhibit only indomethacin-induced ulceration. 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide is
As illustrated by the experimental results shown in Table 3,
It has been proven that it is effective not only for acute treatment. 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) pyrimidine-3-carboxamide,
The procedure for these experiments was similar to that for the acute experiments, except that a dose of 50 mg/Kg was administered orally for 4 consecutive days. Injury agent (ethanolic hydrochloric acid or 0.6 molar hydrochloric acid) was administered on day 4 and the experiment was evaluated as described for the acute experiment. 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide is
Even those caused by ethanolic hydrochloric acid or 0.6 molar hydrochloric acid could provide a protective effect against the development of significant changes. Not only the frequency of ulcers but also their number and severity decreased. Ulceration occurred in each animal in the control group. On the other hand, 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Less severe ulcers were observed in only 60 or 80% of the animals treated with pyrimidine-3-carboxamide. Protective action and recovery of advanced injuries occur not only in the stomach, but also in other parts of the gastrointestinal system.
1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Given by pyrimidine-3-carboxamide. Effect on ulcer formation in the intestines, 10
In a group of Sprague-Dawley CFY mice,
The cases of cimetidine and atropine were compared and studied. It is also of great importance to know whether compounds that inhibit gastric mucosal injury can also inhibit intestinal ulceration. If gastric mucosal injury is only suppressed, then
Intestinal ulcers become perforated [British Journal of Permanent Colology (British J.Pham.)
67, 33 (1979)]. Similar to the experiments described above, indomethacin was used as the ulcerating agent. Compounds under study (cimetidine, astropine,
1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Each of the pyrimidine-3-carboxamides was administered to the animals for 4 consecutive days, while the ulcerative agent (indomethacin) was given once on the second day. During the experiment, the animals had free access to food and water. After 4 days, the animal was killed, the abdomen was incised, and the injury to the gastrointestinal system was removed using the Tsumori method [J.Pharm.D. 3, 659]
-660 (1980)]. The ulcer is
Scoring was performed according to the ulceration index as follows. Intact mucous membrane 0 1-3 small ulcers or sores 1 1-5 ulcers or sores 2 More than 5 ulcers or 1-3 perforated ulcers 3 Many perforated ulcers 4 Observation of dead animals or Besides observing the length of the small intestine from the pylorus to the cecum, the animals' weight and frequency of ascites were also measured. The first control group did not receive any protective or ulcerative agents. A second control group received only the ulcerating agent, namely indomethacin. A third control group received ulcerative agents and cimetidine. On the other hand, the fourth control group
Astropine was given in addition to ulcerative agents. The fifth control group was 1,6-dimethyl-4-oxo-
1,6,7,8,9,9a-hexahydro-4H-
This gave pyrido(1,2-a)pyrimidine-3-carboxamide. The sixth group received 1,6-dimethyl-4-oxo-1,6,7,8,9,9a- in addition to ulcerative agents for 4 days.
Hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide was obtained. The results of these experiments are summarized in Table 4. 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide was protected with respect to all variables investigated. It can be concluded that it can only have a positive effect. The protective effect of astropine was less obvious. Furthermore, 1,6-dimethyl-4-oxo-1,
The protective effect of 6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide was investigated in acute and 4-day experiments with pure ethanol without hydrochloric acid. The induced gastric ulcer formation was studied. The results are shown in Table 5. In acute experiments, 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-
4H-pyrido(1,2-a)pyrimidine-3-carboxamide was administered orally to Sprague-Dawley CFY mice 40 minutes prior to oral administration of 0.5 ml of ethanol. During the four consecutive days of the experiment, the animals received 1,6-
dimethyl-4-oxo-1,6,7,8,9,
9a-hexahydro-4H-pyrido (1,2-a)
Pyrimidine-3-carboxamide was given orally for 4 consecutive days and 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexa-hydro-4H-pyrido ( The administration of 1,2-a) pyrimidine-3-carboxamide was followed by oral administration of 0.5 ml of ethanol 40 minutes later. The antiulcer effect was measured in both experiments 2 hours after administration of the ulcerative agent. The severity of ulceration was scored as follows. Intact mucous membrane 0 Ulcer or erosion 1-2 mm long 1 Ulcer 2-3 mm long 2 Ulcer 3-4 mm long 3 Ulcer longer than 4 mm 4 Thick ulcer longer than 4 mm 5 As shown in Table 5 , 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3-
Carboxamide inhibited ethanol-induced gastric ulcer formation not only after 4 days of treatment but also in acute experiments. (Effect) To summarize in Tables 2 to 5, 1,6-dimethyl-4
-Oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-
It is clear that the 3-carboxamide was the only drug that had a protective and prophylactic effect on the entire gastrointestinal system, whereas the effects of both cimetidine and atropine, used as controls, were similar to those of the injurious drug. It was only involved in the protection of the stomach. (Effect of the invention) According to the present invention, 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-
4H-pyrido(1,2-a)pyrimidine-3-carboxamide is produced by chemical or other exogenous and endogenous agents, either by using prophylactic or therapeutic methods. It provides protection and recovery for the entire gastrointestinal system against injury. The treatment is carried out with commonly used pharmaceutical compositions such as tablets, capsules, dragees, suppositories, injections containing about 10 to 1000 mg of active ingredient, depending on the type of formulation. Whether to use once or divided doses per day will depend on the patient's condition, age, severity of injury, and method of use. Daily oral dosage varies between 100 and 1000 mg. Depending on the severity of the developed injury, parenteral, especially subcutaneous, intradermal, or intravenous drug therapy may also be used. Daily intravenous doses vary between 10 and 400 mg. For subcutaneous administration, doses of 20-800 mg are given. [Table] [Table] [Table] [Table] [Table] [Table] [Table] (Example) Examples of the present invention are illustrated in detail by the following non-limiting examples. Example 1 Preparation of tablets each containing 100 mg of active ingredient 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide 1000
A mixture containing 300 g of lactose and 300 g of lactose was sieved to homogenize, and the powdered mixture was then moistened with 200 ml of a 5% aqueous gelatin solution. After drying and re-granulation,
The granules are treated with stearic magnesium phosphate salt.
20 g of talcum, 40 g of talc and 40 g of potato starch and then compressed into tablets. Example 2 Preparation of tablets each containing 200 mg of active ingredient 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide 2000
A mixture containing g and 600 g of potato starch was sieved to homogenize, then this powdered mixture was
Wet with 300 ml of 5% aqueous gelatin solution. After drying and regranulation, the granules were homogenized with a powder mixture containing 40 g of talc, 30 g of magnesium stearate, and 30 g of potato starch and then compressed into tablets. Example 3 Preparation of tablets each containing 300 mg of active ingredient 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide 3000
Sift a mixture containing 300g of potato starch and 300g of potato starch to make it homogeneous.
ml of 5% aqueous gelatin solution. After drying and regranulation, the granules were homogenized with a powder mixture containing 120 g of talc, 50 g of magnesium stearate and 30 g of potato starch and then compressed into tablets. Example 4 Preparation of sugar-coated tablets containing 100 mg, 200 mg, and 300 mg of the active ingredient 1,6-dimethyl-4-oxo-1,6,7,8,9,9a- A pigment suspension was used to coat tablets containing hexahydro-4H-pyrido(1,2-a)pyrimidine-3-carboxamide. A fine powder mixture containing 64 g of talcum and 50 g of titanium dioxide was homogenized with 268 g of isopropanol. water
4g water-soluble dye and 6000 carbo wax in 12g
A colored aqueous solution containing 6 g was prepared and mixed with the suspension prepared above. The medicinal suspension thus obtained was used to coat the surface of 1000 tablets. Example 5 Preparation of injection solution (2ml/100g) (2ml/100g)
g) 1,6-dimethyl-4-oxo-1,6,7,
8,9,9a-hexahydro-4H-pyrido (1,
2-a) Pyrimidine-3-carboxamide 1000
g was weighed in a 2 volume volumetric flask and dissolved in water used for injection. After completely dissolving 20% in water for injection, it was prepared and filtered through a glass filter to make it transparent. 2 ml of the resulting solution was sterilized at 120℃ for 30 minutes.
Filled into voluminous glass bottles. Example 6 Preparation of suppositories containing 200 mg of active ingredient 50 g of colloidal silicon hydroxide material is added to the suppository base
g, and liquefied (adepus solidus) at 40-45°C. 1,6-dimethyl-4-oxo-1,6,7,8,9,9a- with a particle size of 10Ό
A 200 g amount of hexahydro-4H-pyrido(1,2-a)pyrimidine was suspended with a small amount of liquefied suppository base with constant stirring. The suspension was mixed with the required supplementary amount of solid fat liquefaction and filled into graduated suppository molds to obtain 1000 suppositories with an average weight of 2.5 g. Example 7 Preparation of a dry syrup containing 100 mg/5 ml of active ingredient A homogeneous mixture containing 156 g of sucrose and 240 g of cocoa powder is mixed with 0.25 g of methyl-p-hydroxybenzoate and propyl-p-hydroxybenzoic acid as preservatives. 0.35g of salt, vanillin as an aromatizer
Added 0.40g. Then 1,6-dimethyl-4-
Oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine-3
- 20 g of carboxamide were weighed out to this powder mixture, homogenized again and sieved. Before use, the mixture was filled to 1000 g with water.

Claims (1)

【特蚱請求の範囲】  ラセミ䜓の又は光孊的掻性の−ゞメチ
ル−−オキ゜−9a−ヘ
キサヒドロ−4H−ピリド−ピリミ
ゞン−−カルボキシアミドの有効量を含有する
こずを特城ずする朰瘍の治療及び予防甚薬剀。  朰瘍が胃腞の朰瘍である特蚱請求の範囲第
項蚘茉の薬剀。  朰瘍が胃朰瘍又は小腞朰瘍である特蚱請求の
範囲第項蚘茉の薬剀。  朰瘍が、胃腞に埓来の消炎剀を摂取するこず
によ぀お生じる朰瘍である特蚱請求の範囲第項
蚘茉の薬剀。  朰瘍が゚タノヌルの摂取によ぀お生じる朰瘍
である特蚱請求の範囲第項蚘茉の薬剀。[Scope of Claims] 1 Racemic or optically active 1,6-dimethyl-4-oxo-1,6,7,8,9,9a-hexahydro-4H-pyrido(1,2-a)pyrimidine - A drug for treating and preventing ulcers, comprising an effective amount of 3-carboxamide. 2 Claim 1 in which the ulcer is a gastrointestinal ulcer
Drugs listed in section. 3. The drug according to claim 1, wherein the ulcer is a gastric ulcer or a small intestinal ulcer. 4. The drug according to claim 1, wherein the ulcer is an ulcer caused by ingesting a conventional anti-inflammatory agent in the stomach and intestines. 5. The drug according to claim 1, wherein the ulcer is an ulcer caused by ingestion of ethanol.
JP60252590A 1984-11-12 1985-11-11 Therapy Granted JPS61171420A (en)

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
HU2251-4192/84 1984-11-12
HU419284 1984-11-12

Publications (2)

Publication Number Publication Date
JPS61171420A JPS61171420A (en) 1986-08-02
JPH0351688B2 true JPH0351688B2 (en) 1991-08-07

Family

ID=10967278

Family Applications (1)

Application Number Title Priority Date Filing Date
JP60252590A Granted JPS61171420A (en) 1984-11-12 1985-11-11 Therapy

Country Status (5)

Country Link
US (1) US4666912A (en)
EP (1) EP0182569B1 (en)
JP (1) JPS61171420A (en)
AT (1) ATE72115T1 (en)
DE (1) DE3585312D1 (en)

Families Citing this family (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
HU201551B (en) * 1988-02-03 1990-11-28 Chinoin Gyogyszer Es Vegyeszet Process for producing 4-oxo-4h-pyrido(1,2-a)pyrimidine-3-carboxylic acid amide derivatives and pharmaceutical compositions comprising same
DE19904392A1 (en) 1999-02-04 2000-08-10 Bayer Ag Polycarbonate molding compounds with improved antistatic properties
DE10050662A1 (en) 2000-10-13 2002-04-18 Gruenenthal Gmbh New substituted dihydropyrido-pyrimidine derivatives, useful for treating e.g. pain, urinary incontinence and tinnitus

Family Cites Families (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
HU174901B (en) * 1976-06-25 1980-04-28 Chinoin Gyogyszer Es Vegyeszet Process for preparing new pyrido /1,2-a/pyrimidine derivatives

Also Published As

Publication number Publication date
EP0182569A2 (en) 1986-05-28
US4666912A (en) 1987-05-19
EP0182569A3 (en) 1987-10-14
EP0182569B1 (en) 1992-01-29
JPS61171420A (en) 1986-08-02
DE3585312D1 (en) 1992-03-12
ATE72115T1 (en) 1992-02-15

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